연간 결과 및 전략적 옵션 검토
25 4월 2024
데스티니 파마 plc
("Destiny Pharma" or "the company")
Audited results for the year ended 31 December 2023 and commencement of review of strategic options to support advancement of XF-73 nasal programme
브라이튼, 영국 - Destiny Pharma plc (AIM: DEST), a clinical stage innovative biotechnology company focused on the development of novel medicines that can prevent life threatening infections, announces its audited financial results for the year ended 31 December 2023. The company also announces the commencement of a review of strategic options to support the company's advancement of XF-73 nasal through Phase 3 clinical trials.
운영 하이라이트
XF-73 nasal - taking steps to maximise value
· Engaging with a number of potential partners regarding a licencing deal
o Positive feedback received from various parties regarding the commercial appeal of XF-73 nasal
o In response to the feedback received to date, the company is developing a new clinical trial design that would, subject to regulatory review, more than halve the previously planned Phase 3 trial costs (post-period)
· Confirmed significant commercial potential and establishing US Go-To-Market model (post-period)
· Data from largest study to date on XF‐73 published in 세포 및 감염 미생물학의 개척자 demonstrated effectiveness of XF‐73 against all 2,527 tested antibiotic resistant and sensitive bacterial strains obtained from patient infections
· Landmark Phase 2b clinical data for XF-73 nasal gel in cardiac surgery patients demonstrating primary endpoint was met (significant reduction in nasal bacteria prior to surgery) published in leading US peer reviewed journal, 감염 관리 및 병원 역학
NTCD-M3 - secured collaboration and co-development deal and enhanced competitive profile
· Partnering deal agreed with Sebela Pharmaceuticals covering North America (US, Canada, and Mexico) worth up to $570m plus royalties; Sebela responsible for financing all remaining clinical development and North America commercialisation
· Strengthened CMC programme on NTCD-M3 to deliver clinical and commercial product supply and transition from liquid to solid dose, strengthening competitive profile; Sebela to conduct a further Phase 2 study following market research confirming the commercial preference for a solid dose oral formulation (post-period)
· Peer reviewed paper published in 미생물학 스펙트럼 concludes that NTCD-M3 is effective alongside all currently recommended antibiotics, including fidaxomicin, in the treatment of CDI
Earlier stage pipeline - focused development of further commercial opportunities
· Enhanced understanding of the potential commercial opportunity of the XF pipeline with early data (antibacterial & anti-fungal)
· Encouraging data demonstrating superior efficacy of XF-73 compared to a leading topical antibiotic against MRSA in skin infection models published in 감염 및 약물 저항성
· Preclinical data in NIAID XF-73 dermal funded study supporting the safety profile and efficacy against a broad range of disease-relevant and antibiotic resistant bacterial isolates (post-period); announced intention to progress towards clinical evaluation for the treatment of diabetic foot infections (DFI) and serious burn wound infections, two areas with a clear unmet need and large patient populations (post-period)
· Discontinued the SPOR-COV development collaboration to focus on potentially higher-value core pipeline assets (post-period)
강화된 이사회 및 경영진
· Board strengthened with the appointments of Chris Tovey, CEO, and Sir Nigel Rudd, Chair
· Dr Debra Barker resumed her position as a Non-Executive Director and assumed the role of CMO on an interim basis
재무 하이라이트
· Loss before tax reduced to £6.4 million (2022: £7.7 million)
· R&D 지출 3.3만 파운드(2022년: 4.9만 파운드)
· Other operating expenses (excluding share-based payment charge) of £3.8 million (2022: £2.5 million)
· 연말 현금 및 현금 등가물 6.4만 파운드(2022년: 4.9만 파운드)
· Company funded through to Q1 2025.
XF-73 nasal update - review of strategic options to advance the programme
The company today provides an update regarding licencing for XF-73 nasal. The company has engaged with a number of potential partners and has received some strong and positive feedback on XF-73 nasal. However, no potential licencing deal has, to date, been forthcoming that we believe would provide fair value to the company and its shareholders.
Destiny Pharma believes the commercial appeal of this asset is very clear, however feedback from potential partners has highlighted their desire for further clarification regarding the cost of Phase 3 clinical trials and prevailing perceptions of the commercial potential of antibiotics. Destiny Pharma has therefore taken steps to re-evaluate aspects of the final clinical development approach to act on this feedback and enhance the attractiveness of XF-73 nasal. These steps include developing a new clinical trial design that, subject to regulatory review, would more than halve the previously anticipated Phase 3 trial costs without reducing XF-73 nasal's market potential, label, or benefits to patients. Further, the company is conducting an ongoing exercise to broaden understanding of the market potential for XF-73 nasal in the US to present potential partners with a clearer, more-in-depth picture of the product's value as a preventative treatment, and how commercial organisations can realise this value. With the benefit of this enhanced proposition, the company will continue to engage with interested parties.
Whilst licencing activities continue, Destiny Pharma believes that it is appropriate to evaluate alternative options to maximise value from XF-73 nasal and progress the programme. To that end, the Board and management are now undertaking a review of strategic options to determine how best to support the company's advancement of XF-73 nasal through Phase 3 clinical trials.
This review will consider a range of strategic options for XF-73 nasal, including licensing and the company securing finance to enable it to conduct the Phase 3 clinical studies. Currently, the review is not actively considering an offer for the company. A further announcement regarding the outcome of this review will be provided in due course.
Chris Tovey, Chief Executive Officer of Destiny Pharma, commented:
"In the eight months since I joined Destiny, everything I have seen and heard furthers my belief in the value our pipeline can bring to patients and health systems around the world. XF-73 nasal has enormous market potential and can make a huge difference in the prevention of surgical site infections, and the reduction in the usage of antibiotics.
'Whilst we will now be presenting an enhanced proposition for the product to potential partners, we also have initiated a wider review to evaluate a range of strategic options to progress the programme and to maximise value from XF-73 nasal. We have a team with a strong track record of bringing products to market and I believe that we can bring this expertise to bear to give XF-73 nasal and Destiny Pharma the best chance of success."
웹 캐스트
Destiny Pharma will host a webcast presentation followed by a live Q&A session at 11:00 am BST today, accessible via the Investor Meet Company platform.
프레젠테이션은 애널리스트와 모든 기존 및 잠재적 신규 주주에게 열려 있습니다.
투자자는 Investor Meet Company에 무료로 가입하고 다음을 통해 Destiny Pharma plc에 추가할 수 있습니다.
https://www.investormeetcompany.com/destiny-pharma-plc/register-investor. Investors who already follow Destiny Pharma plc on the Investor Meet Company platform will automatically be invited.
자세한 내용은 문의하시기 바랍니다 :
데스티니 파마 plc
크리스 토비, CEO
숀 클레이던, CFO
+44 (0)1273 704 440
FTI 컨설팅
벤 앳웰 / 사이먼 콘웨이 / 마이클 트레이스
+ 44 (0) 203 727 1000
쇼어 캐피탈(지명 고문 및 Broker)
다니엘 부시 / 제임스 토마스 / 루시 보든
+ 44 (0) 207 408 4090
데스티니 파마 소개
Destiny Pharma is an innovative, clinical-stage biotechnology company focused on the development and commercialisation of novel medicines that can prevent life-threatening infections. The company's drug development pipeline includes two late-stage assets XF-73 nasal gel, a proprietary drug targeting the prevention of post-surgical staphylococcal hospital infections including MRSA and NTCD-M3, a microbiome-based biotherapeutic for the prevention of C. difficile infection (CDI) recurrence which is the leading cause of hospital acquired infection in the US.
회사에 대한 자세한 내용을 보려면 다음 사이트를 방문하세요. www.destinypharma.com이 발표에 포함된 정보는 시장 남용(개정)(EU 출구) 규정(SI 596)에 따라 영국 국내법의 일부인 시장 남용 규정(EU) 번호 2014/2019에 규정된 내부 정보를 구성하는 것으로 간주됩니다. /310) ("영국 XNUMX월"). 이 발표가 발표되면 이 내부 정보(UK MAR에 정의됨)는 이제 공개 영역에 있는 것으로 간주됩니다.
미래 예측 진술
Certain information contained in this announcement, including any information as to the company's strategy, plans or future financial or operating performance, constitutes "forward-looking statements". These forward looking statements may be identified by the use of forward-looking terminology, including the terms "believes", "estimates", "anticipates", "projects", "expects", "intends", "aims", "plans", "predicts", "may", "will", "seeks" "could" "targets" "assumes" "positioned" or "should" or, in each case, their negative or other variations or comparable terminology, or by discussions of strategy, plans, objectives, goals, future events or intentions. These forward-looking statements include all matters that are not historical facts. They appear in a number of places throughout this announcement and include statements regarding the intentions, beliefs or current expectations of the Directors concerning, among other things, the company's results of operations, financial condition, prospects, growth, strategies and the industries in which the company operates. The Directors of the company believe that the expectations reflected in these statements are reasonable but may be affected by a number of variables which could cause actual results or trends to differ materially. Each forward-looking statement speaks only as of the date of the particular statement. By their nature, forward-looking statements involve risks and uncertainties because they relate to events and depend on circumstances that may or may not occur in the future or are beyond the company's control. Forward looking statements are not guarantees of future performance. Even if the company's actual results of operations, financial condition and the development of the industries in which the company operates are consistent with the forward-looking statements contained in this document, those results or developments may not be indicative of results or developments in subsequent periods.
최고 경영자의 성명서
Operational and review of strategic options for XF-73 nasal
Destiny Pharma has two lead assets which have both successfully completed Phase 2 and have been shown to be effective and well tolerated. They act through two completely different mechanisms, reducing the risk in the pipeline through clear diversification.
We believe that XF-73 nasal, the lead drug candidate from our XF platform, has a target product profile that is very attractive to surgeons and hospital infection experts. There are many millions of hospital operations in the US alone where a new drug is needed to help prevent post-surgical infections.
Our other lead drug candidate, NTCD-M3, for the prevention of CDI, is focused on infection prevention and very well positioned as a targeted, naturally occurring bacterial therapy for this serious gut infection. The NTCD-M3 programme positions the company in the exciting area of the human microbiome and biotherapeutics, which is a fast-developing area of medical science and investigation for new therapies.
XF 플랫폼
The XF platform is delivering several exciting research and clinical programmes focusing on infection prevention with the potential to deliver not only patient benefits, but also clear cost savings to healthcare systems across the world, whilst delivering safe, effective anti-infective treatments that also address the issue of antimicrobial resistance ("AMR").
XF를 뒷받침하는 임상 데이터-73 코 프로그램이 강하다
The positive Phase 2b results announced in 2021 confirmed the potential of XF-73 nasal gel. XF-73 (exeporfinium chloride) was awarded Qualified Infectious Disease Product ("QIDP") status by the FDA. Within the QIDP award, the FDA also confirmed a new US disease indication for XF-73 nasal; namely the "prevention of post-surgical staphylococcal infections", including MRSA. This represents a potential new US indication for which no existing product is approved.
Destiny Pharma has now completed seven successful clinical trials in over 300 subjects with XF-73 nasal gel, which included measures of its efficacy in reducing nasal colonisation by Staphylococcus aureus.
2년에 완료된 2021b상 연구는 멀티-센터, 무작위, 위약-controlled study of multiple applications of a single concentration of XF-73 nasal gel to assess the antimicrobial effect of XF-73 nasal gel on commensal Staphylococcus aureus nasal carriage in patients scheduled for surgical procedures.
Destiny Pharma's experience in carrying out this clinical study has confirmed the increasing compliance in US hospitals with best practice, whereby patients are screened, and carriers of Staphylococcus aureus are decolonised, prior to surgery. This is very supportive of the potential sales in the initial market for XF-73 nasal gel in the large US hospital surgery market.
외과적 감염과 싸우기 위한 의학적 필요성이 중요합니다.
Patient carriage of Staphylococcus aureus strains, including MRSA, is recognised as a growing problem and the testing of patients entering hospital for surgery is widespread in many countries, including the US.
In Europe, similar guidelines exist recommending decolonisation of Staphylococcus aureus positive patients prior to certain surgeries.
The antibiotic mupirocin is often used off-label in the US for these applications, although it has two key disadvantages in that it is slow acting, requiring five days of dosing, and staphylococcal resistance to mupirocin develops rapidly and can become widespread. Consequently, many guidelines are accompanied with a resistance warning related to mupirocin use. In 2020 another new review concluded that global mupirocin-resistant Staphylococcus aureus prevalence had increased to 7.6% and that mupirocin-resistant MRSAs have increased by 13.8% and consequently the monitoring of mupirocin use remains critical. Destiny Pharma believes this is clear support for the need for an alternative treatment for nasal decolonisation as presented by XF-73 nasal, which has no observed bacterial (MRSA) resistance to date. (Ref. Mupirocin Resistance in Staphylococcus aureus: A Systematic Review and Meta-Analysis - Dadashi et al 2020).
Phase 3 study designs for XF-73 nasal
Destiny Pharma is developing a new clinical trial design, which builds upon previous engagement with the key regulators in the US and Europe, that, we believe, will more than halve the previously planned Phase 3 trial costs. The new clinical trial design maintains the previous target indication and commercial opportunity. The company is engaged in a comprehensive partnering campaign with the aim of finding one or more partners to enable the progression to Phase 3 study, in 2025.
The proposed plan is to carry out two Phase 3 randomised, double-blind, placebo-controlled clinical trials in patients undergoing two different surgical procedures. The planned studies could deliver a data set that would support the preferred, broad label for XF-73 nasal gel, supporting its use in all major surgeries as a novel treatment delivering fast, effective prevention of post-surgical Staphylococcal infections. This would be the first approval of a product for this indication, which creates both significant differentiation from other products, and access to a very large commercial opportunity.
The commercial opportunity for XF-73 nasal
The Board believes that XF-73 nasal gel can be priced competitively across the world, has both excellent efficacy against a wide range of gram-positive bacteria especially 황색 포도상 구균 (including MRSA), has an excellent safety profile and addresses the key challenge of AMR.
The market analysis undertaken by Destiny Pharma and its specialist consultants supports the view that XF-73 nasal could achieve annual peak sales in the US alone of over $1 billion and peak sales in Europe and the rest of the world could also be significant for the initial indication of "prevention of post-surgical staphylococcal infections".
XF 연구 프로그램
During the period under review, the company has continued to work on several projects looking at the activity of the XF platform in selected infection models, including the activity of XF compounds against bacteria and fungi embedded in biofilms. The company also entered new research projects testing XF compounds in models of oral mucositis and cystic fibrosis, the latter research project being supported by a funding award from the Cystic Fibrosis Foundation. The continuing research work adds to the understanding of the XF platform's novel mode of action and helps identify potential new opportunities to develop targeted research projects that may lead to new clinical development opportunities for the XF platform. The company will continue to seek grant and other non-dilutive funding support for these earlier-stage research projects as it has done with some success, with approximately £3.5 million in grant funding secured since the IPO in 2017.
NTCD-M3 Clostridioides difficile programme
NTCD-M3 was developed by GI infection physician Professor Dale Gerding, who is a world-leading specialist in C. difficile, with more than 400 peer-reviewed journal publications, book chapters and review articles in the area. NTCD-M3 has successfully completed Phase 1 and Phase 2b trials. The Phase 2b study demonstrated a strong safety/toxicology profile and 95% prevention of CDI recurrence. Phase 2b NTCD-M3 data was published in the prestigious Journal of the American Medical Association (Gerding DN et al JAMA 2015;313:1719).
NTCD-M3 has also been awarded Fast Track status by the FDA. Destiny Pharma acquired global rights to the NTCD-M3 programme in November 2020 and in 2023 out-licensed the programme to Sebela Pharmaceuticals (US, Canada and Mexico) who will fund all the remaining required clinical development including Phase 3 studies and lead commercialisation in North America.
NTCD-M3 mechanism of action harnesses the human microbiome
NTCD-M3 is a naturally occurring non-toxigenic strain of C. difficile bacteria, which lacks the genes that can express C. difficile toxins. It is an oral formulation of NTCD-M3 spores and patients who have taken NTCD-M3 were found to be protected from C. difficile infections. NTCD-M3 acts as a safe "ground cover" preventing toxic strains of C. difficile proliferating in the colon after antibiotic treatment. NTCD-M3 temporarily colonises the human gut without causing any symptoms and the gut microbiome returns to normal a few weeks after treatment.
The Phase 2 data from a completed study with NTCD-M3, conducted with a liquid formulation, was very promising. The study was a randomised, double-blind, placebo-controlled trial, among 173 patients aged >18 years, who were diagnosed as having CDI (either a first episode or first recurrence). The results were a strong, statistically significant data set showing rapid onset of colonisation which provided protection during the early post-treatment period, making it an ideal complement to a vaccine and other antibiotic treatments. The rate of recurrence ("RR") of CDI after treatment with the best dose of NTCD-M3 was only 5% (placebo 30%), p<0.01. The company believes this is compelling efficacy compared with clinical trial data from other approaches.
Prior to signing the collaboration and co-development agreement with Sebela, the company held discussions with the FDA as part of Type C meetings and this clarified the minimum work required to prepare for Phase 3 clinical trials, including the Phase 3 design and certain manufacturing scale-up activities.
During 2023, the company has reviewed the chemistry, manufacturing and controls (CMC) programme for NTCD-M3. Following this review, the company changed its contract development manufacturing organisation for NTCD-M3 in order to strengthen manufacturing for clinical trial material and improve future commercial supply. In doing so, this supports the necessary transition of NTCD-M3 from a liquid to a solid dose formulation, which, based on market research with physicians and patients is the preferred formulation, and therefore further strengthens the competitive profile of NTCD-M3. As a result of these changes, Sebela Pharmaceuticals intend to conduct a small Phase 2 study to create new data on the solid dose formulation and de-risk the Phase 3 study. Sebela has the right, at its own cost, to complete any further trials. The company is working with Sebela through the joint steering committee to accelerate the development plan to commercialisation.
In 2024 the plan is to complete the necessary manufacturing process development to enable the production of product for clinical trial supply and to strengthen manufacturing for future commercial supply. Following this, our partner, Sebela Pharmaceuticals, can then initiate the next stage of clinical development in 2025.
SPOR-COV
Following the period end we notified SporeGen of our intention not to extend our collaboration development after it concludes in April 2024, as we focus resources on development of the XF platform and our other key company pipeline programmes.
데스티니 파마에 대한 전망
Destiny Pharma will continue to progress along its course to become a world-leading, anti-infective company that develops products that play both an important role in protecting vulnerable patients across the world from potential lethal infections and achieves commercial success.
Given the significant opportunity that it presents, management will be focused on securing progression of XF-73 nasal into Phase 3 study as quickly as possible. Destiny Pharma is developing a new clinical trial design, which builds upon previous engagement with the key regulators in the US and Europe, that, we believe, will more than halve the previously planned Phase 3 trial costs. The new clinical trial design maintains the previous target indication and commercial opportunity. To enable Destiny Pharma to capitalise on the significant and important potential of XF-73 nasal, the Board are now undertaking a review of strategic options for XF-73 nasal to determine how best to support the company's advancement of the programme.
The partnering deal for NTCD-M3 announced with Sebela demonstrates that management are able to deliver on the company's strategy and are able to find partners to support the development of the company's key assets through the final stages of development to approval and commercialisation. Management will continue to look at opportunities to strengthen the programme to enhance commercial competitiveness such as the shift to a solid dose oral presentation.
Additionally, cash resources are also being used to progress the exciting pipeline candidates from the pre-clinical XF pipeline, with the XF-73 dermal programme being the most important. Whilst the short-term focus is clearly on our two highly valuable lead assets, Destiny Pharma will continue to establish research programmes through existing and new collaborations and, where possible, seek additional non-dilutive funding support as it has done successfully in the period under review.
Destiny Pharma has a great opportunity as a focused UK biotechnology company, listed on AIM, with two high-quality, late-stage clinical assets targeted at infection prevention. Both are backed up by strong Phase 2 clinical data and have clear commercial positioning. The Board and employees are excited about the next stage in the company's development and delivering on our strategy to build a world-leading infection prevention company and to build a very valuable company for our shareholders.
크리스 토비
최고 경영자(CEO)
24 4월 2024
최고재무책임자(CFO) 성명서
재무 검토
During 2023 we intensified partnering activities for our lead asset, XF-73 nasal, and completed US market analysis that confirmed the significant market opportunity for this asset of up to $1 billion in the US alone. We also continued to progress the scale-up manufacture required for Phase 3 clinical studies and commercialisation. Our target remains progressing XF-73 nasal into Phase 3 clinical studies as quickly as possible.
We were pleased to announce, in February 2023, an exclusive collaboration and co-development agreement for North American rights for NTCD-M3 with Sebela Pharmaceuticals, a key milestone event for the company. In conjunction with this transaction, we strengthened the company's balance sheet, securing £7.3 million gross proceeds via an equity fundraise from existing and new investors.
The total comprehensive loss for the year was £5.7 million (2022: £6.5 million).
At 31 December 2023 the company had cash and cash equivalents totalling £6.4 million (2022: £4.9 million), providing a cash runway until Q1 2025. Details of the Directors' assessment on going concern is provided in note 3 to the financial statements.
수익
Destiny Pharma is a clinical stage research and development company and is yet to commercialise and generate sales from its current programmes. During the year, the company received £0.8 million of licence fee income by way of an upfront payment from Sebela Pharmaceuticals, under its exclusive collaboration and co-development agreement for NTCD-M3 (2022: £nil).
운영 비용
Operating expenses, which exclude the share-based payment charge of £0.5 million (2022: £0.5 million) during the period, amounted to £7.1 million (2022: £7.4 million). Included within this total are R&D costs totalling £3.3 million (2022: £4.9 million) which were £1.6 million lower than the prior year. This was largely due to the re-phasing of manufacturing costs for our NTCD-M3 programme. We successfully transitioned to a new CDMO for the programme in the second half of the year and are pleased with progress since the change.
Other operating costs increased by 51% to £3.8 million (2022: £2.5 million). Other operating costs are split between general overheads, which increased by £1.1 million to £2.2 million (2022: £1.1 million), and employee costs, which increased by £0.2 million to £1.6 million (2022: £1.4 million). During the year, one-off operating costs were incurred in relation to changes to the Board, as we strengthened the leadership team, and completing the Sebela transaction. We also increased spend on business development activities, including completing US market analysis for XF-73 nasal.
과세
The company received a repayment of £1.2 million in respect of the R&D tax credit claimed during the year ended 31 December 2022. The R&D tax credit receivable in the balance sheet of £0.8 million is an estimate of the cash repayment the company expects to qualify for in respect of activities during the year ended 31 December 2023. However, as at the date of this report, these amounts have not yet been agreed with HMRC.
현금 흐름
Net cash outflow from operating activities in 2023 was £5.5 million (2022: £5.9 million) against an operating loss of £6.7 million (2022: £7.8 million), with the major reconciling items being the non-cash charge for share-based payments of £0.5 million, the R&D credit received of £1.2 million and net movements in working capital of £(0.4) million.
Net cash from financing activities during the year of £6.7 million represents the net proceeds of the equity fundraise in the first quarter of 2023 (2022: £6.1 million). The net increase in cash and cash equivalents during the period was £1.5 million (2022: increase of £0.3 million).
대차 대조표
Total assets increased to £10.0 million (2022: £8.8 million), largely due to a higher cash and cash equivalents compared to the prior year.
Intangible assets comprise the initial acquisition cost of NTCD-M3, acquired in November 2020, and a milestone payment to NTCD LLP of £0.1 million following completion of the Sebela transaction. Other receivables, and prepayments decreased to £1.2 million (2022: £1.6 million), which was primarily due to a lower R&D tax credit compared to the prior year.
Year-end cash and cash equivalents totalled £6.4 million (2022: £4.9 million.
Total liabilities decreased to £0.8 million (2022: £1.2 million), primarily due to lower accrued development costs at the year end compared to the prior year.
숀 클레이던
최고 재무담당자(CFO)
24 4월 2024
포괄 손익 계산서
31년 2023월 XNUMX일로 종료되는 연도에 대해
| 연말 | 연말 | |
|
| 31 12월 | 31 12월 |
|
| 2023 | 2022 |
| 노트 | £ | £ |
지속적인 운영 |
|
|
|
라이센스 수수료 수입 | 7 | 831,552 | - |
기타 영업 수입 |
| - | 154,499 |
관리비 |
| (7,092,067) | (7,397,014) |
주식기준보상비용 |
| (475,479) | (533,829) |
운영 손실 |
| (6,735,994) | (7,776,344) |
금융 수입 | 5 | 289,756 | 64,800 |
세전 손실 |
| (6,446,238) | (7,711,544) |
과세 | 6 | 789,202 | 1,207,975 |
계속영업손실 및 당기총포괄손실 |
| (5,657,036) | (6,503,569) |
주당 손실 - 펜스 |
|
|
|
Basic | 8 | (6.2:XNUMX)p | (9.3:XNUMX)p |
희석 | 8 | (6.2:XNUMX)p | (9.3:XNUMX)p |
재무상태표
31 년 2023 월 XNUMX 일 기준
| ~에서 | ~에서 | |
|
| 31 12월 | 31 12월 |
|
| 2023 | 2022 |
| 노트 | £ | £ |
자산 |
|
|
|
비유동 자산 |
|
|
|
재산, 식물 및 장비 |
| 19,235 | 24,621 |
무형 자산 | 9 | 2,341,469 | 2,261,435 |
비유동 자산 |
| 2,360,704 | 2,286,056 |
유동 자산 |
|
|
|
기타 채권 | 10 | 899,725 | 1,410,452 |
선불 |
| 314,452 | 195,814 |
현금 및 현금성 자산 | 11 | 6,382,603 | 4,903,461 |
유동 자산 |
| 7,596,780 | 6,509,727 |
총자산 |
| 9,957,484 | 8,795,783 |
자산 및 부채 |
|
|
|
공평 |
|
|
|
주식 자본 | 12 | 952,719 | 733,071 |
프리미엄 공유 |
| 39,568,625 | 33,043,569 |
누적 손실 |
| (31,332,176) | (26,150,619) |
주주 지분 |
| 9,189,168 | 7,626,021 |
유동 부채 |
|
|
|
매입 채무 및 기타 채무 | 13 | 768,316 | 1,169,762 |
유동 부채 |
| 768,316 | 1,169,762 |
총 지분 및 부채 |
| 9,957,484 | 8,795,783 |
자본변동표
31년 2023월 XNUMX일로 종료되는 연도에 대해
공유 | 공유 | 누적 된 |
| |
| 자본 | 프리미엄 | 사상자 수 | 금액 |
| £ | £ | £ | £ |
1월 1 2022 | 598,719 | 27,091,466 | (20,180,879) | 7,509,306 |
올해 종합 적자 |
|
|
|
|
총 포괄 손실 | - | - | (6,503,569) | (6,503,569) |
해당 연도의 총 포괄 손실 | - | - | (6,503,569) | (6,503,569) |
소유자에 의한 기부 및 분배 |
|
|
|
|
자본금 발행 | 134,352 | 6,332,565 | - | 6,466,917 |
주식 발행 비용 | - | (380,462) | - | (380,462) |
주식기준보상비용 | - | - | 533,829 | 533,829 |
소유자의 총 기부금 및 소유자에 대한 분배 | 134,352 | 5,952,103 | 533,829 | 6,620,284 |
31 12월 2022 | 733,071 | 33,043,569 | (26,150,619) | 7,626,021 |
올해 종합 적자 |
|
|
|
|
총 포괄 손실 | - | - | (5,657,036) | (5,657,036) |
해당 연도의 총 포괄 손실 | - | - | (5,657,036) | (5,657,036) |
소유자에 의한 기부 및 분배 |
|
|
|
|
자본금 발행 | 219,648 | 7,127,065 | - | 7,346,713 |
주식 발행 비용 | - | (602,009) | - | (602,009) |
주식기준보상비용 | - | - | 475,479 | 475,479 |
소유자의 총 기부금 및 소유자에 대한 분배 | 219,648 | 6,525,056 | 475,479 | 7,220,183 |
31 12월 2023 | 952,719 | 39,568,625 | (31,332,176) | 9,189,168 |
현금 흐름표
31년 2023월 XNUMX일로 종료되는 연도에 대해
연말 | 연말 | |
| 31 12월 | 31 12월 |
| 2023 | 2022 |
| £ | £ |
영업 활동으로 인한 현금 흐름 |
|
|
소득세 전 손실 | (6,446,238) | (7,711,544) |
유형 자산의 감가 상각 | 6,196 | 12,328 |
주식기준보상비용 | 475,479 | 533,829 |
금융 수입 | (289,756) | (64,800) |
| (6,254,319) | (7,230,187) |
기타채권 및 선급금의 (증가)/감소 | (26,684) | 14,316 |
(감소)/매매대금 및 기타채무의 증가 | (401,446) | 396,326 |
영업에 사용된 현금 | (6,682,449) | (6,819,545) |
받은 세금 | 1,207,975 | 927,256 |
영업 활동에 사용 된 순 현금 | (5,474,474) | (5,892,289) |
투자 활동으로 인한 현금 흐름 |
|
|
부동산, 플랜트 및 장비 구매 | (810) | (1,067) |
무형 자산 매입 | (80,034) | - |
받은이자 | 289,756 | 64,800 |
투자활동으로 인한 순현금유입 | 208,912 | 63,733 |
금융 활동으로 인한 현금 흐름 |
|
|
순 발행 비용을 차감한 신주 발행 | 6,744,704 | 6,086,455 |
재무활동으로 인한 순현금유입 | 6,744,704 | 6,086,455 |
현금 및 현금 등가물의 순증가 | 1,479,142 | 257,899 |
연초의 현금 및 현금성자산 | 4,903,461 | 4,645,562 |
현금 및 현금성자산 연말정산 | 6,382,603 | 4,903,461 |
재무제표에 대한 주석
1. 일반 정보
Destiny Pharma plc (the "company") was incorporated and domiciled in the UK on 4 March 1996 with registration number 03167025. The company's registered office is located at Unit 36, Sussex Innovation Centre, Science Park Square, Falmer, Brighton BN1 9SB.
The company is engaged in the discovery, development and commercialisation of novel medicines that prevent serious infections.
2. 준비의 기초
The financial statements have been prepared in accordance with UK-adopted International Accounting Standards. The financial statements have been prepared under the historical cost convention except where stated otherwise within the accounting policies.
회사의 재무제표는 회사의 기능 및 표시 통화인 파운드 스털링("GBP")으로 표시됩니다.
3. 관심가는
The company has not yet recorded any sales revenues and funds its operations through periodic capital issues, commercial partnerships and research grants. Management prepares detailed working capital forecasts which are reviewed by the Board on a regular basis. These forecasts consider sensitivities on receipts and costs. Based on the Directors' current forecasts the company's current cash runway is forecast to extend until Q1 2025 at which point a further capital injection would be required.
The Directors continue to evaluate all options to fund the development of its assets in a way that realises maximum value whilst meeting the future needs of the company, including continuing discussions with a number of potential partners for its lead assets. However, there is no guarantee that attempts to secure adequate cash inflows from commercial partnerships or through equity fund raising or other sources within the timescales stated above will be successful. These conditions indicate the existence of a material uncertainty, which may cast significant doubt about the company's ability to continue as a going concern.
The Directors have a reasonable expectation that the company will be able to secure the necessary funds to have adequate cash resources to continue to meet the requirements of the business. Accordingly, the Board continues to adopt the going concern basis in preparing the financial statements.
4. 세그먼트 보고
최고 운영 의사 결정자는 회사의 이사회로 간주됩니다. 최고운영의사결정자는 자원을 할당하고 영업부문 수준에서 사업성과 및 기타 활동을 평가합니다.
최고 운영 의사 결정자는 회사가 제약 제제의 개발 및 상업화라는 하나의 운영 부문을 가지고 있다고 결정했습니다. 모든 활동은 영국에서 이루어집니다.
5. 순금융수익
31 12월 2023 £ | 31 12월 2022 £ | |
금융 수입 |
|
|
입금계좌이자 | 289,756 | 64,800 |
6. 소득세
31 12월 2023 £ | 31 12월 2022 £ | |
회계 연도의 비용을 기준으로 한 연구 개발 세액 공제 | (789,202) | (1,207,975) |
7. Licence fee income
31 12월 2023 £ | 31 12월 2022 £ | |
라이센스 수수료 수입 | 831,552 | - |
Licence fees for the year ended 31 December 2023 comprise an upfront payment of $1 million (£0.8 million) received from Sebela Pharmaceutical® ("Sebela") relating to the exclusive collaboration and co-development agreement ("licensing agreement") for NTCD-M3, signed in February 2023.
8. 보통주당손실
해당 기간의 보통주(기본주 및 희석주)당 손실은 해당 기간 동안 주주에게 귀속되는 법인세 후 이익을 기준으로 계산됩니다. 당기 중 손실이 발생하여 희석성 잠재적보통주가 발행되지 않아 기본주당손실과 희석주당손실이 동일합니다. 계산은 다음과 같습니다.
31 12월 2023 £ | 31 12월 2022 £ | |
당기 주주 귀속 손실 | (5,657,036) | (6,503,569) |
가중평균주식수 | 90,671,329 | 70,182,231 |
주당 손실 - 펜스 |
|
|
- 기본 및 희석 | (6.2:XNUMX)p | (9.3:XNUMX)p |
9. 무형자산
획득 한 개발 프로그램 £ | |
비용 |
|
1년 2022월 XNUMX일 | 2,261,435 |
추가 | - |
31년 2022월 XNUMX일 | 2,261,435 |
추가 | 80,034 |
31년 2023월 XNUMX일 | 2,341,469 |
2020년에는 균종 독성 예방을 위한 개발 단계 프로그램인 NTCD-M3를 인수했다. C. 디피 실리 proliferating in the colon after antibiotic treatment. Consideration payable by the company for the asset is made up of an upfront payment, development milestones, sales royalties and sales milestones. The upfront payment was recognised as an addition in 2020.
In February 2023, the company signed an exclusive collaboration and co-development agreement ("licensing agreement") for NTCD-M3 with Sebela Pharmaceuticals. This licencing agreement triggered a milestone payment of $100,000 (£80,034) under the company's agreement to acquire the NTCD-M3 programme. This is included as an addition in 2023.
The asset has not been amortised as the programme has not yet generated products available for commercial use.
The programme has been assessed for impairment. The company considers the future development costs, the probability of successfully progressing to product approval and the likely commercial returns, among other factors. The result of this assessment did not indicate any impairment in the year.
The key sensitivity for all development programmes is the probability of successful completion of clinical trials in order to obtain regulatory approval for sale. Should trials be unsuccessful, the programme will be fully impaired.
10. 기타채권
31 12월 | 31 12월 | |
| 2023 | 2022 |
| £ | £ |
기타 채권 | 110,523 | 202,477 |
연구개발 세금 환급 | 789,202 | 1,207,975 |
| 899,725 | 1,410,452 |
11. 현금 및 현금성자산
31 12월 2023 £ | 31 12월 2022 £ | |
현금 및 은행 잔고 | 2,704,395 | 1,903,461 |
콜 보증금 | 3,678,208 | 3,000,000 |
현금 및 현금성 자산 | 6,382,603 | 4,903,461 |
12. 자본금 공유
각 £0.01의 보통주 | 31 12월 2023 번호 | 31 12월 2022 번호 |
인정 받은(1) | N / A | N / A |
할당 및 전액 지불 |
|
|
1월 XNUMX일 | 73,307,105 | 59,871,921 |
연중 현금으로 발행 | 21,964,758 | 13,435,184 |
31월 XNUMX일 | 95,271,863 | 73,307,105 |
(1) During the year ended 31 December 2017 the company adopted new Articles of Association, which do not require the company to have authorised share capital.
| 31 12월 2023 £ | 31 12월 2022 £ |
인정 받은 | N / A | N / A |
할당 및 전액 지불 | 952,719 | 733,071 |
| 31 12월 2023 £ | 31 12월 2022 £ |
프리미엄 계정 공유 | 39,568,625 | 33,043,569 |
21,294,758주의 보통주가 £7,127,065의 프리미엄으로 해당 연도에 발행되었습니다. 당해 연도 중 주식 프리미엄에 부과된 주식 발행 비용은 £602,009였습니다.
각 보통주는 의결권, 배당금 및 분배, 청산 시 자본 반환에 대해 파리 파수 순위를 매깁니다.
옵션 부여
On 12 May 2023, 213,854 Employee LTIP 2020 options were granted to four employees at an exercise price of £0.01 per ordinary share. The fair value per option was £0.33.
On 12 May 2023, 217,500 Employee LTIP 2018 options were granted to twelve employees at an exercise price of £0.35 per ordinary share. The fair value per option was £0.26.
On 18 November 2023, 3,053,532 Employee LTIP 2020 options were granted to three employees at an exercise price of £0.01 per ordinary share. The fair value per option was £0.29.
주식선택권의 행사가격과 가중평균행사가격은 다음과 같습니다.
| 31 12월 2023 | 31 12월 2022 | ||
| 수 옵션 | 가중 평균 운동 가격 | 수 옵션 | 가중 평균 운동 가격 |
연초에 미결제 잔액 | 8,868,230 | £0.115 | 9,759,125 | £0.112 |
연도 중 부여 | 3,484,886 | £0.031 | 244,282 | £0.360 |
연중 행사 | (1,002,802) | £0.010 | (526,177) | £0.024 |
연도 중 경과 | (1,684,502) | £0.170 | (609,000) | £0.248 |
연말에 뛰어난 옵션 | (9,665,812) | £0.087 | 8,868,230 | £0.115 |
연말에 행사 가능한 옵션 | 5,615,320 | £0.063 | 5,800,049 | £0.035 |
31년 2023월 6.1일 현재 미결제 주식 옵션의 가중 평균 잔여 계약 만기는 2022년(4.3년: XNUMX년)이었습니다.
당기에 인식한 주식기준보상거래에서 발생한 비용은 다음과 같습니다.
| 31 12월 2023 £ | 31 12월 2022 £ |
주식기준보상비용 | 475,479 | 533,829 |
13. 매출채권 및 기타채무
| 31 12월 2023 £ | 31 12월 2022 £ |
매입 채무 | 395,428 | 172,543 |
사회 보장 및 기타 세금 | 70,262 | 80,369 |
미지급 비용 | 299,243 | 898,326 |
납부 가능한 연금 기여금 | 3,383 | 18,524 |
| 768,316 | 1,169,762 |
14. 법정계정
The financial information set out above does not constitute the company's statutory accounts for the year ended 31 December 2023 but is derived from those accounts. The audit report on those accounts was unqualified but drew attention to a material uncertainty related to going concern. The report did not contain a statement under section 498 (2) or (3) of the Companies Act 2006. The statutory accounts for the year ended 31 December 2023 have not yet been filed at Companies House.
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